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Cell Mol Neurobiol. Author manuscript; available in PMC 2011 March 14.
Published in final edited form as:
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David S. Goldstein
Clinical Neurocardiology Section, Clinical Neurosciences Program, Division of Intramural
Research, National Institute of Neurological Disorders and Stroke, National Institutes of Health,
Building 10, Room 5N220, 9000 Rockville Pike, 10 Center Drive, MSC-1620, Bethesda, MD
20892-1620, USA
Abstract
Based on concepts proposed by Langley, Cannon, and Selye, adrenal responses to stress occur in a
syndrome that reflects activation of the sympathoadrenal system and hypothalamic–pituitary–
adrenocortical (HPA) axis; and a “stress syndrome” maintains homeostasis in emergencies such as
“fight or flight” situations, but if the stress response is excessive or prolonged then any of a variety
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of clinical disorders can arise. The idea of a unitary sympathoadrenal system does not account for
evidence that different stressors elicit different patterns of autonomic responses, with exposure to
some stressors differentially affecting sympathetic noradrenergic and adrenomedullary hormonal
activities. Instead, adrenomedullary responses to stressors are more closely tied to adrenocortical
than to sympathetic noradrenergic responses. Distress involves concurrent activation of the HPA
and adrenomedullary neuroendocrine systems.
Keywords
Stress; Adrenal; Epinephrine; Norepinephrine; Sympathetic nervous system
Cannon taught that noxious environmental or internal stimuli threatening homeostasis (e.g.,
exposure to cold, hypotensive hemorrhage, traumatic pain, insulin-induced hypoglycemia,
emotionally distressing antagonistic encounters) concurrently activate the adrenal gland to
release epinephrine (EPI, synonymous with adrenaline) and the sympathetic nervous system.
He considered the two effectors to function as a unit, which came to be termed the
“sympathoadrenal,” “sympathico-adrenal,” of “sympathoadrenomedullary” system. In
emergencies, sympathoadrenal activation would tend to restore homeostasis. Indeed, in
1939, Cannon formally and erroneously proposed that the chemical messenger of the
sympathetic nervous system was identical to EPI (Cannon and Lissak 1939). Cannon
emphasized that disparate threats to homeostasis incite the same sympathoadrenal response
(Cannon 1929b, 1939). The notion of a unitary sympathoadrenal system continues in
medical thinking (Cryer 1980; Shah et al. 1984; Sofuoglu et al. 2001; Kvetnansky et al.
1995).
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Selye proposed three universal stages of coping with a stressor—the “General Adaptation
Syndrome”—an initial “alarm reaction,” analogous to Cannon’s “fight or flight” response, a
stage of adaptation, with resistance to the stressor, and eventually a stage of exhaustion and
organismic death. In Selye’s early experiments, after injection of any of a variety of tissue
extracts or of formalin into rats, the animals developed a pathological triad of enlargement
of the adrenal glands, atrophy of lymphoid tissue in the thymus, spleen, and lymph nodes,
and bleeding gastrointestinal ulcers. It was later demonstrated that these changes are
associated with and to at least some extent result from activation of the HPA axis. Steroids
released into the circulation from the adrenal cortex are required for resistance but are also
responsible for pathological changes. Selye’s concept that prolonged stress can produce
disease is now widely accepted.
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Selye acknowledged that responses to stressors have a specific component that tends to
counter effects of the stressor; however, after removal of specific responses from
consideration, a non-specific stress syndrome would remain. Chrousos and Gold (1992)
modified Selye’s doctrine of non-specificity by proposing that above a threshold intensity,
any stressor elicits the stress syndrome.
More than a half century elapsed before Selye’s doctrine of non-specificity underwent
experimental testing, which failed to confirm it (Pacak et al. 1998). Even so, modern lay and
even scientific literature continues to accept the notions of a unitary stress response, a
central neural stress system, and a stress “syndrome.” For instance, a Google search yielded
about 4,000,000 hits for “the stress response,” 714,000 hits for “the stress system,” and
202,000 for “the stress syndrome.”
Modern concepts view stress as a sensed threat to homeostasis (McEwen and Stellar 1993;
Goldstein and McEwen 2002), in which the response has a degree of specificity depending
on the particular challenge to homeostasis and the organism’s perceptions of the stressor and
ability to cope with it (Goldstein 2001).
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Homeostats
Central to scientific integrative medicine in general and to systems concepts of stress
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Homeostatic systems operate according to a few principles that despite their simplicity can
explain complex physiological phenomena and might help resolve controversial issues in the
area of stress and disease.
Positive feedback loops are inherently unstable, and conversion from a negative to a positive
neurocirculatory feedback loop presages rapid decompensation. For instance, one can
understand transitions from heat stress to heat shock and from compensated to
decompensated heart failure in terms of positive feedback loops (Goldstein 2006).
Multiple Effectors
Multiple effectors regulate levels of most monitored variables of the body (Fig. 2). Having
available multiple effectors extends the range of control, allows at least some regulation of
the monitored variable if a particular effector fails (compensatory activation), and enables
elaboration of specific, adaptive effector patterns.
the sympathetic nervous system acts only as an “emergency” system (Gauthier et al. 1972;
Julien et al. 1990).
Effector Sharing
Different homeostatic systems can interact by sharing effectors (Fig. 3). This can help
understand clinical associations that might otherwise be unexpected. For instance, sharing of
the adrenomedullary hormonal system by the barostat and glucostat can explain
hyperglycemia in gastrointestinal hemorrhage, and sharing of the vasopressin system by the
barostat and osmostat can explain hyponatremia in heart failure.
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Primitive Specificity
Beginning soon after adequately sensitive assay methods of plasma levels of norepinephrine
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(NE) and EPI became available, evidence rapidly accumulated for different noradrenergic
versus adrenergic responses in different situations (Cryer 1980; Robertson et al. 1979;
Young and Landsberg 1979; Young et al. 1984). These findings did not fit with the notion of
a unitary sympathoadrenal system.
In the sheltered confines of a laboratory, with controlled temperature and ad libitum water,
nutrients, and calories, mammals do not seem to require an intact sympathetic nervous
system (Cannon 1931). It is by now clear that even under resting conditions pulse-
synchronous bursts of skeletal muscle sympathetic nerve activity are detectable, and NE
continuously enters the venous drainage of most organs. Activities of daily life, such as
standing up (Lake et al. 1976), digesting a meal (Patel et al. 2002), speaking in public (Gerra
et al. 2001), and walking—i.e., not only emergencies—are associated with rapid adjustments
in sympathetic nervous system outflows.
Adrenomedullary hormonal system activity, and thereby EPI levels, respond to global or
metabolic threats, such as hypoglycemia, hemorrhagic hypotension, exercise beyond an
anaerobic threshold, asphyxiation, emotional distress, and shock. Evidence also has
accumulated for an association between NE and active escape, avoidance, or attack, and an
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association between EPI and passive, immobile fear. Thus, in contrast with Selye’s doctrine
of non-specificity, according to the systems theory of stress activities of effector systems are
coordinated in relatively specific neuroendocrine patterns.
Studies of humans exposed to cold or with mild core hypothermia have provided support for
the notion of primitive specificity of neuroendocrine stress responses. Cold exposure
increases plasma NE levels, with little if any increases in plasma EPI or ACTH levels,
consistent with sympathetic neuronal activation and relatively less adrenomedullary and
adrenocortical activation. Mild core hypothermia also increases antecubital venous levels of
NE but not EPI (Frank et al. 2002). Both NE and EPI levels in arterial plasma increase in
this setting, but with larger NE responses (Goldstein and Frank 2001). When these
homeostatic mechanisms are overwhelmed and core temperature falls, then increased
adrenomedullary secretion results in high circulating EPI levels, increasing generation of
calories (Staten et al. 1987) and eliciting cutaneous vasoconstriction, which decreases
evaporative heat loss. The adrenomedullary activation is associated with distress, which
motivates escape and avoidance learning.
Allostasis
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Homeostasis implies set goal values for monitored variables; however, ranges of acceptable
values are decidedly inconstant. Levels of physiological activity required to re-establish or
maintain homeostasis differ, depending on continually changing conditions in which the
organism finds itself—e.g., running versus standing versus lying down. “Allostasis,” a term
used by Sterling and Eyer in 1988 (McEwen 1998), refers to levels of activity required for
the individual to “maintain stability through change”—i.e., to adapt (McEwen 1998, 2000;
Schulkin et al. 1998). Regulation around an altered apparent steady state is the essence of
allostasis. Adaptations involving allostasis to cope with real, simulated, or imagined
challenges are determined by genetic, developmental, and experiential factors.
Homeostat resetting redefines the conditions required to maintain homeostasis. This would
be analogous to a different thermostatic setting in the winter compared to the summer. A
neuroendocrine example is the hyperglycemia of exercise. Even in anticipation of the need
for metabolic fuel, by activation of “central command,” the blood glucose level increases to
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Resetting alters activities of multiple effector systems required to maintain allostasis, at least
for short durations. During stress, short-term changes in homeostatic settings generally
enhance the long-term well-being and survival of the organism. When superimposed on a
substrate of pathology, however, homeostatic resetting can cause harm. For instance, in the
setting of ischemic heart disease, global or patterned increases in sympathetic outflows from
homeostat resetting would increase cardiac work, and the resulting imbalance between
oxygen supply and demand could precipitate angina pectoris, myocardial infarction, or
sudden death.
Allostatic Load
While they may be effective over a short interval, allostatic alterations may have cumulative
long-term adverse effects. For instance, chronic elevation of blood pressure to ensure
adequate blood flow to the brain might eventually lead to heart or kidney failure. “Allostatic
load” (McEwen and Stellar 1993) refers to effects of prolonged continuous or intermittent
activation of effectors involved in allostasis. In the analogy of the home temperature control
system, allostatic load would increase if a window or door were left open. In this situation,
one or more effectors might be activated frequently or even continuously. Long-term
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allostatic load—the wear and tear cost of adaptation—provides a conceptual basis for
studying long-term health consequences of stress (Fig. 4).
Chronic effector system activation might alter the efficiency of the homeostatic system
itself. For instance, chronic sympathetic nervous stimulation of the cardiovascular system
could promote cardiovascular hypertrophy, “splinting” arterial baroreceptors in stiff blood
vessel walls, in turn contributing to systolic hypertension and the risk of heart failure, kidney
failure, and stroke. Moreover, an inappropriately large adrenomedullary response to a
stressor might exaggerate the experience of distress (Schachter and Singer 1962).
Exaggerated distress responses might increase the risk of worsening an independent
pathologic process, such as in panic-induced angina pectoris (Wilkinson et al. 1998;
Mansour et al. 1998).
Recently, panels of specific indices have been proposed as biomarkers of allostatic load
(Juster et al. 2010). Because of the primitive specificity of stress response patterns, one
might question the universal applicability of such panels. On the other hand, in chronic
distress, a set of indices might reflect consequences of persistent activation of the adrenal
cortex and medulla.
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Thus, one way of looking at stress is as a condition where expectations, whether genetically
programmed, established by prior learning, or deduced from circumstances, do not match
current or anticipated perceptions of the internal or external environment, and this
discrepancy between what is observed or sensed and what is expected or programmed elicits
patterned, compensatory responses (Fig. 4).
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without separating these two very different characteristics. The systems theory of stress does
not assume an equivalence of noxiousness (i.e., negatively reinforcing properties) with
production of pathological changes; that is, the theory does not assume that distress causes
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disease.
Selye’s theory emphasized the non-specificity of the stress response, whereas according to
the systems theory, the experience of distress depends on the character, intensity, and
meaning of the stressor as perceived by the organism and on the organism’s perceived
ability to cope with it. This is in line with Lazarus’s views on emotional stress and
psychological coping (Somerfield and McCrae 2000). For an organism to experience
distress therefore seems to require consciousness, to interpret the situation in terms of the
ability to cope. This notion can help explain the finding that sedation with the
benzodiazepine, alprazolam, attenuates the ACTH and EPI responses to glucoprivation
(Breier et al. 1992).
Distress responses, as all stress responses, have a “purpose,” mitigating effects of a stressor
in some way. This applies not only to neuroendocrine aspects of those responses (such as the
glucose counter-regulatory actions of pituitary-adrenocortical and adrenomedullary
stimulation during insulin-induced hypoglycemia) but also to psychological aspects (such as
conditioned aversive and instrumental avoidance learning).
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Distress responses evolved and continue to be expressed even in higher organisms, including
humans who actually are only rarely exposed to truly “fight-or-flight” agonistic encounters,
partly because of the importance of those responses in instinctive communication. Selye’s
theory did not consider the communication function of distress.
A recent study based on computer searches of PubMed (Goldstein and Kopin 2008)
retrieved publications describing original data about plasma EPI, ACTH, and NE levels
measured before and during or after exposure to stressors. Magnitudes of responses were
categorized according to the following criteria. If there was no significant change in plasma
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levels of the dependent variable, a score of 0 was assigned. If there were a statistically
significant increase but less than a doubling of the pre-stress baseline level, a score of 1 was
assigned. If there were at least a doubling of the baseline value, up 3 times the baseline
value, a score or 2 was assigned. If there were a large increase, from 3 up to 10 times the
baseline value, a score of 3 was assigned. If there was a massive increase to ≥10 times the
baseline value, a score of 4 was assigned. A total of 15 different stressors were identified for
which the available literature satisfied the above criteria.
Mean EPI responses were strongly positively correlated with mean ACTH responses (Fig. 5)
and less strongly with NE responses. Plasma EPI responses were larger than expected for
NE responses during hypoglycemia and smaller than expected for NE responses during cold
exposure with-out hypothermia, orthostasis, and active escape/avoidance. Plasma NE
responses were larger than expected for ACTH responses during cold exposure without
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hypothermia and severe/exhausting exercise and smaller than expected for ACTH responses
during hypoglycemia.
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Thus there seems to be at least as good a justification for the concept of coordinated
adrenocortical–adrenomedullary responses as for coordinated adrenomedullary–
sympathoneural responses in stress. This coordination may involve corticotropin releasing
hormone driving adrenocortical and adrenomedullary outflows (Yoshida-Hiroi et al. 2002)
as well as interactions between adrenocortical and adrenomedullary chromaffin cells
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Fig. 1.
A physiological homeostatic system. As the level of the monitored variable changes,
afferent information is compared with a set point or other algorithm for responding, and the
sensed discrepancy leads to altered activities of effectors. Note the odd number of (–) signs,
indicating a negative feedback loop. In response to a continuous perturbation, the level of
the monitored variable reaches an apparent steady state
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Fig. 2.
Compensatory activation. One advantage of multiple effectors is compensatory activation of
alternative effectors if one effector fails, enabling control of the monitored variable. For
instance, thyroidectomy augments sympathetic nervous system (SNS) responses to cold
exposure
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Fig. 3.
Effector sharing. Sharing of an effector by multiple homeostats can explain unpredicted
consequences and syndromic features of disease processes. For instance, in heart failure,
decreased aortic filling increases levels of vasopressin (AVP), which, as the antidiuretic
hormone, promotes retention of free water, explaining hyponatremia attending heart failure
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Fig. 4.
Systems definitions of stress and allostatic load. In stress, the organism senses a discrepancy
between afferent information about a monitored variable and a set point and other
instructions for responding, altering activities of effectors to decrease the discrepancy.
Allostatic load reflects wear and tear, which, if sustained and substantial enough, decreases
effector efficiency, further activating the effector and accelerating wear and tear. Allostatic
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load can therefore eventuate in a destabilizing and pathologic positive feedback loop
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Fig. 5.
Mean values across 15 different stressors for plasma levels of a epinephrine (EPI) and
corticotrophin (ACTH); b EPI and norepinephrine (NE); and c NE and ACTH. Dashed lines
indicate lines of best fit
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Cell Mol Neurobiol. Author manuscript; available in PMC 2011 March 14.